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高度保守的肽基转移酶中心碱基的突变诱导酵母核糖体的补偿性重排。

Mutations of highly conserved bases in the peptidyltransferase center induce compensatory rearrangements in yeast ribosomes.

机构信息

Department of Cell Biology and Molecular Genetics, University of Maryland, College Park, Maryland 20742, USA.

出版信息

RNA. 2011 May;17(5):855-64. doi: 10.1261/rna.2593211. Epub 2011 Mar 25.

Abstract

Molecular dynamics simulation identified three highly conserved rRNA bases in the large subunit of the ribosome that form a three-dimensional (3D) "gate" that induces pausing of the aa-tRNA acceptor stem during accommodation into the A-site. A nearby fourth base contacting the "tryptophan finger" of yeast protein L3, which is involved in the coordinating elongation factor recruitment to the ribosome with peptidyltransfer, is also implicated in this process. To better understand the functional importance of these bases, single base substitutions as well as deletions at all four positions were constructed and expressed as the sole forms of ribosomes in yeast Saccharomyces cerevisiae. None of the mutants had strong effects on cell growth, translational fidelity, or on the interactions between ribosomes and tRNAs. However, the mutants did promote strong effects on cell growth in the presence of translational inhibitors, and differences in viability between yeast and Escherichia coli mutants at homologous positions suggest new targets for antibacterial therapeutics. Mutant ribosomes also promoted changes in 25S rRNA structure, all localized to the core of peptidyltransferase center (i.e., the proto-ribosome area). We suggest that a certain degree of structural plasticity is built into the ribosome, enabling it to ensure accurate translation of the genetic code while providing it with the flexibility to adapt and evolve.

摘要

分子动力学模拟确定了核糖体大亚基中三个高度保守的 rRNA 碱基,它们形成了一个三维(3D)“门”,在氨酰-tRNA 接受茎适应进入 A 位时诱导其暂停。附近的第四个碱基与参与与肽基转移协同招募延伸因子到核糖体的酵母蛋白 L3 的“色氨酸指”接触,也与该过程有关。为了更好地理解这些碱基的功能重要性,构建了单个碱基取代以及四个位置的缺失,并在酵母酿酒酵母中作为核糖体的唯一形式进行了表达。这些突变体对细胞生长、翻译保真度或核糖体与 tRNA 之间的相互作用都没有强烈影响。然而,突变体在存在翻译抑制剂的情况下确实促进了对细胞生长的强烈影响,并且同源位置的酵母和大肠杆菌突变体之间的生存能力差异表明了新的抗菌治疗靶点。突变体核糖体还促进了 25S rRNA 结构的变化,这些变化都局限于肽基转移酶中心的核心(即原核糖体区域)。我们认为,核糖体中构建了一定程度的结构可塑性,使其能够确保遗传密码的准确翻译,同时为其提供了适应和进化的灵活性。

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